BRD4 Promotes DNA Repair and Mediates the Formation of TMPRSS2-ERG Gene Rearrangements in Prostate Cancer

Li, Xiangyi; Baek, Guem Hee; Ramanand, Susmita G.; Sharp, Adam; Gao, Yunpeng; Yuan, Wei; Welti, Jon; Rodrigues, Daniel Nava; Dolling, David; Figueiredo, Ines; Sumanasuriya, Semini; Crespo, Mateus; Aslam, Adam J.; Li, Rui; Yin, Yi; Mukherjee, Bipasha; Kanchwala, Mohammed; Hughes, Ashley M.; Halsey, Wendy S.; Chiang, Cheng Ming; Xing, Chao; Raj, Ganesh V.; Burma, Sandeep; Bono, Johann S. de; Mani, Ram S.

doi:10.1016/j.celrep.2017.12.078

Cited by 111 publications

(108 citation statements)

References 49 publications

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“…Recently, BET inhibitors have been reported to hamper DNA damage repair through several distinct mechanisms. Li et al . reported that BRD4 participated in NHEJ DNA repair by regulating NHEJ DNA repair genes and interacting with NHEJ DNA repair proteins.…”

Section: Discussionmentioning

confidence: 99%

“…Recently, BET inhibitors have been reported to hamper DNA damage repair through several distinct mechanisms. Li et al 17 reported that BRD4 participated in NHEJ DNA repair by regulating NHEJ DNA repair genes and interacting with NHEJ DNA repair proteins. Wang et al 33 discovered a BRD-like module in the catalytic subunit of DNA-dependent protein kinase (DNA-PKcs-BRD) to which JQ1 could bind and further showed that JQ1 hampered NHEJ DNA repair by impairing DNA-PKcs activity.…”

Section: Discussionmentioning

confidence: 99%

“…Although the effect of BET inhibitors on the expression of oncogenes such as c‐Myc has been extensively addressed, the mechanisms by which BET inhibition produces cytotoxicity remain unknown. However, several recent studies have reported that BRD4 is essential for the repair of DNA double‐strand breaks (DSBs), and that BET inhibitors suppress both of the major DSB repair mechanisms, homologous recombination (HR) and nonhomologous end joining (NHEJ) …”

Section: Introductionmentioning

confidence: 99%

“…However, several recent studies have reported that BRD4 is essential for the repair of DNA double-strand breaks (DSBs), and that BET inhibitors suppress both of the major DSB repair mechanisms, homologous recombination (HR) and nonhomologous end joining (NHEJ). [15][16][17][18] The tyrosine kinase WEE1, which is a crucial component of the G2-M cell cycle checkpoint, prevents mitotic entry in response to cellular DNA damage by acting in cooperation with myelin transcription factor 1 (MYT1) kinase. WEE1 and MYT1 kinases inhibit CDK1 activity by phosphorylating CDK1 at Thr14 and Tyr15, which results in the activation of the G2-M checkpoint and cell cycle arrest.…”

Section: Introductionmentioning

confidence: 99%

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Bromodomain and extraterminal domain inhibition synergizes with WEE1‐inhibitor AZD1775 effect by impairing nonhomologous end joining and enhancing DNA damage in nonsmall cell lung cancer

Takashima

Kikuchi

et al. 2019

Intl Journal of Cancer

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Bromodomain and extraterminal domain (BET) inhibitors are broadly active against distinct types of cancer, including nonsmall cell lung cancer (NSCLC). Previous studies have addressed the effect of BET‐inhibiting drugs on the expression of oncogenes such as c‐Myc, but DNA damage repair pathways have also been reported to be involved in the efficacy of these drugs. AZD1775, an inhibitor of the G2‐M cell cycle checkpoint kinase WEE1, induces DNA damage by promoting premature mitotic entry. Thus, we hypothesized that BET inhibition would increase AZD1775‐induced cytotoxicity by impairing DNA damage repair. Here, we demonstrate that combined inhibition of BET and WEE1 synergistically suppresses NSCLC growth both in vitro and in vivo. Two BET inhibitors, JQ1 and AZD5153, increased and prolonged AZD1775‐induced DNA double‐strand breaks (DSBs) and concomitantly repressed genes related to nonhomologous end joining (NHEJ), including XRCC4 and SHLD1. Furthermore, pharmaceutical inhibition of BET or knockdown of the BET protein BRD4 markedly diminished NHEJ activity, and the BET‐inhibitor treatment also repressed myelin transcription factor 1 (MYT1) expression and promoted mitotic entry with subsequent mitotic catastrophe when combined with WEE1 inhibition. Our findings reveal that BET proteins, predominantly BRD4, play an essential role in DSB repair through the NHEJ pathway, and further suggest that combined inhibition of BET and WEE1 could serve as a novel therapeutic strategy for NSCLC.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Bromodomain and extraterminal domain inhibition synergizes with WEE1‐inhibitor AZD1775 effect by impairing nonhomologous end joining and enhancing DNA damage in nonsmall cell lung cancer

Takashima

Kikuchi

et al. 2019

Intl Journal of Cancer

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“…Immunohistochemistry (IHC) for BRD4, AR-V7 and full length androgen receptor (AR-FL) was performed on patient samples and CP50 PDX as previously described (Supplementary Methods) (25,26,43).…”

Section: Tissue Analysismentioning

confidence: 99%

Targeting Bromodomain and Extra-Terminal (BET) Family Proteins in Castration-Resistant Prostate Cancer (CRPC)

Welti

Sharp

Yuan

et al. 2018

Clinical Cancer Research

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118

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Welti et al; Targeting BET family proteins in CRPC 2 Statement of Translational RelevanceAdvanced prostate cancer invariably progresses to lethal castration resistant prostate cancer (CRPC). Resistance to current androgen receptor (AR) targeting therapies is associated with the development of AR aberrations including the constitutively active AR splice variant 7 (AR-V7). Currently, no clinically available therapies effectively inhibit aberrant AR signaling. BRD4, a bromodomain and extraterminal (BET) family protein, is a critical AR coregulator. We show that BRD4 expression associates with patient outcome and AR driven transcription in lethal prostate cancer. Moreover, BET inhibitors (BETi) reduce AR splicing and AR-V7 expression by regulating alternative splicing, abrogating AR signaling and inhibiting growth of CRPC patient derived models. Clinical studies with BETi in CRPC should pursue pharmacodynamics studies evaluating abrogation of AR splicing and persistent AR signaling to optimize the development of these drugs for the treatment of CRPC.Research. Experimental Design: We determined associations between BET expression, AR driven transcription and patient outcome; and the effect and mechanism by which chemical BETi (JQ1 and GSK1210151A; I-BET151) and BET family protein knockdown regulates AR-V7 expression and AR signaling in prostate cancer (PC) models.Results: Nuclear BRD4 protein expression increases significantly (p=<0.01) with castration resistance in same patient treatment naïve (median H-score; interquartile range: 100; 100-170) and CRPC (150; 110-200) biopsies, with higher expression at diagnosis associating with worse outcome (HR 3.25, 95% CI 1.50-7.01; p=<0.001). BRD2, BRD3 and BRD4 RNA expression in CRPC biopsies correlates with AR driven transcription (all p=<0.001). Chemical BETi, and combined BET family protein knockdown, reduce AR-V7 expression and AR signaling. This was not recapitulated by C-MYC knockdown. In addition, we show that BETi regulates RNA processing thereby reducing alternative splicing and AR-V7 expression. Furthermore, BETi reduce growth of PC cells and patient derived organoids with known AR mutations, AR amplification and AR-V7 expression. Finally, BETi, unlike enzalutamide, decreases persistent AR signaling and growth (p=<0.001) of a patient derived xenograft model of CRPC with AR amplification and AR-V7 expression. Conclusion:BETi merit clinical evaluation as inhibitors of AR splicing and function, with trials demonstrating their blockade in proof of mechanism pharmacodynamic studies.

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BRD4 in physiology and pathology: ‘‘BET’’ on its partners

Liang

Tian

2021

BioEssays

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Bromodomain-containing 4 (BRD4), a member of Bromo and Extra-Terminal (BET) family, recognizes acetylated histones and is of importance in transcription, replication, and DNA repair. It also binds non-histone proteins, DNA and RNA, contributing to development, tissue growth, and various physiological processes. Additionally, BRD4 has been implicated in driving diverse diseases, ranging from cancer, viral infection, inflammation to neurological disorders. Inhibiting its functions with BET inhibitors (BETis) suppresses the progression of several types of cancer, creating an impetus for translating these chemicals to the clinic. The diverse roles of BRD4 are largely dependent on its interaction partners in different contexts. In this review we discuss the molecular mechanisms of BRD4 with its interacting partners in physiology and pathology. Current development of BETis is also summarized. Further understanding the functions of BRD4 and its partners will facilitate resolving the liabilities of present BETis and accelerate their clinical translation.

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BRD4 Promotes DNA Repair and Mediates the Formation of TMPRSS2-ERG Gene Rearrangements in Prostate Cancer

Cited by 111 publications

References 49 publications

Bromodomain and extraterminal domain inhibition synergizes with WEE1‐inhibitor AZD1775 effect by impairing nonhomologous end joining and enhancing DNA damage in nonsmall cell lung cancer

Bromodomain and extraterminal domain inhibition synergizes with WEE1‐inhibitor AZD1775 effect by impairing nonhomologous end joining and enhancing DNA damage in nonsmall cell lung cancer

Targeting Bromodomain and Extra-Terminal (BET) Family Proteins in Castration-Resistant Prostate Cancer (CRPC)

BRD4 in physiology and pathology: ‘‘BET’’ on its partners

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